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靶向登革病毒部分非结构蛋白 3 的 C5a 受体促进黏膜登革疫苗模型中抗原特异性 IFN-γ 产生的 T 细胞应答。

C5a receptor targeting of partial non-structural protein 3 of dengue virus promotes antigen-specific IFN-γ-producing T-cell responses in a mucosal dengue vaccine model.

机构信息

Department of Molecular Biology and the Institute for Molecular Biology and Genetics, Chonbuk National University, Jeonju 54896, Republic of Korea.

Department of Bioactive Material Sciences and Research Center of Bioactive Materials, Chonbuk National University, Jeonju 54896, Republic of Korea.

出版信息

Cell Immunol. 2018 Mar;325:41-47. doi: 10.1016/j.cellimm.2018.01.016. Epub 2018 Feb 15.

Abstract

Mucosal vaccination is an ideal strategy to induce protective immunity in both mucosal and parenteral areas. Successful induction of an antigen-specific immune response via mucosal administration essentially requires the effective delivery of antigen into a mucosal immune inductive site, which depends on antigen delivery into M cells. We previously reported that M cells specifically express C5aR, and antigen targeting to C5aR by using specific ligands, including Co1 peptide, promotes the antigen-specific immune response in both mucosal and systemic immune compartments. In this study, we found that application of the Co1 peptide to dengue virus antigen containing CD8 T cell epitopes effectively induced an antigen-specific IFN-γ-producing CD8 T cell response after oral mucosal administration of antigen. Consequently, we suggest that Co1 peptide-mediated C5aR targeting of antigen into M cells can be used for the induction of an effective antigen-specific CD8 T cell immune response in oral mucosal vaccine development.

摘要

黏膜免疫接种是诱导黏膜和全身部位保护性免疫的理想策略。通过黏膜给予成功诱导抗原特异性免疫应答,本质上需要将抗原有效递送至黏膜免疫诱导部位,这取决于抗原递送至 M 细胞。我们之前报道过 M 细胞特异性表达 C5aR,并且通过使用特异性配体(包括 Co1 肽)将抗原靶向 C5aR,可促进黏膜和全身免疫区室中的抗原特异性免疫应答。在这项研究中,我们发现将 Co1 肽应用于含有 CD8 T 细胞表位的登革热病毒抗原,可在经口黏膜给予抗原后有效诱导抗原特异性 IFN-γ 产生的 CD8 T 细胞应答。因此,我们认为 Co1 肽介导的 C5aR 将抗原靶向 M 细胞,可用于诱导口腔黏膜疫苗开发中有效的抗原特异性 CD8 T 细胞免疫应答。

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